Affinage

Showing MACO1TMEM57 is a alias.

MACO1

Macoilin · UniProt Q8N5G2

Length
664 aa
Mass
76.2 kDa
Annotated
2026-06-10
17 papers in source corpus 8 papers cited in narrative 8 extracted findings
Cross-family judge faithfulness: 5/5 claims corpus-supported (100%)

Mechanistic narrative

Synthesis pass · prose summary of the discoveries below

MACO1 (macoilin/TMEM57) encodes a conserved multi-transmembrane protein of the rough endoplasmic reticulum that is expressed broadly and specifically in the nervous system, where it controls neuronal excitability and sensory signaling (PMID:21437263, PMID:21589894). In C. elegans, loss of maco-1 produces presynaptic neurotransmission defects (aldicarb resistance, levamisole sensitivity) and abolishes the rising-O2 Ca2+ response of the PQR sensory neuron in a manner mirroring mutation of the L-type voltage-gated Ca2+ channel α1 subunit egl-19, supporting a model in which macoilin acts within the ER to regulate the assembly or trafficking of ion channels or their regulators (PMID:21437263). ER localization and a neuronal function are conserved: human MACO1 localizes to the rough ER and weakly rescues the thermotaxis defect of maco-1 mutants, which themselves show altered thermosensory Ca2+ responses in AFD and AIY neurons (PMID:21589894). Through this control of sensory Ca2+ dynamics, MACO-1 acts downstream of the TIR-1/JNK-1 pathway to promote recovery of attenuated odor-evoked responses, thereby driving forgetting of olfactory adaptation, and is also required for pheromone-induced dauer formation (PMID:28924007, PMID:26976437). Independently, maco-1 is the molecular endpoint of a trans-kingdom small-RNA silencing mechanism: small RNAs from Pseudomonas species (PA14-derived P11; P. vranovensis Pv1) bear complementarity to maco-1 and downregulate it via the RNAi/piRNA pathway to drive learned, transgenerationally inherited pathogen avoidance, a circuit in which maco-1 acts downstream of or parallel to the VAB-1 receptor (PMID:32908307, PMID:38547071, PMID:40267186).

Mechanistic history

Synthesis pass · year-by-year structured walk · 7 steps
  1. 2011 High

    Established macoilin as a neuron-specific rough-ER protein whose loss disrupts presynaptic function and sensory Ca2+ responses, generating the model that it regulates ion channel assembly/trafficking from the ER.

    Evidence Fluorescent localization, in vivo Ca2+ imaging of PQR, aldicarb/levamisole pharmacology, and genetic epistasis with egl-19/nca-1/nca-2 in C. elegans

    PMID:21437263

    Open questions at the time
    • No direct biochemical demonstration that macoilin binds or chaperones EGL-19 or other channels
    • Mechanism distinguishing assembly versus trafficking not resolved
  2. 2011 High

    Demonstrated cross-species conservation of ER localization and neuronal function, showing human MACO1 can substitute for the worm protein in thermotaxis.

    Evidence Subcellular localization, cross-species rescue by human MACO1 expression, and Ca2+ imaging of AFD/AIY neurons

    PMID:21589894

    Open questions at the time
    • Rescue was only weak/partial
    • Human MACO1 molecular activity not directly assayed in a mammalian system
  3. 2016 Medium

    Placed MACO-1 in pheromone signaling by showing it is required for ascaroside-pheromone-induced dauer formation.

    Evidence Forward EMS genetic screen and dauer formation assays in C. elegans

    PMID:26976437

    Open questions at the time
    • No molecular mechanism linking MACO-1 to pheromone detection/integration
    • Site of action within the dauer pathway undefined
  4. 2017 High

    Connected MACO-1 to a defined signaling pathway by showing it acts downstream of TIR-1/JNK-1 to promote recovery of sensory Ca2+ responses and forgetting of olfactory adaptation.

    Evidence Forward suppressor screen, double-mutant epistasis, in vivo Ca2+ imaging, and histamine-gated chloride channel neuronal silencing

    PMID:28924007

    Open questions at the time
    • How ER-localized MACO-1 mechanistically restores Ca2+ response recovery is unknown
    • Relationship between this role and channel trafficking not established
  5. 2020 High

    Identified maco-1 as the silencing target of a bacterial non-coding small RNA, defining it as the genetic endpoint of a trans-kingdom RNAi/piRNA pathway driving heritable pathogen avoidance.

    Evidence PA14 sRNA purification and feeding, RNAi knockdown, loss-of-function genetics, and behavioral/transgenerational assays with RNAi/piRNA pathway epistasis

    PMID:32908307

    Open questions at the time
    • How reduced MACO-1 in specific neurons translates to avoidance behavior not mechanistically resolved
    • Link between ER/channel function and avoidance circuit not established
  6. 2024 High

    Generalized the sRNA-targeting mechanism by showing a distinct Pseudomonas species uses an independent small RNA (Pv1) complementary to maco-1 to induce heritable avoidance.

    Evidence Bacterial sRNA sequencing, sRNA deletion/rescue for necessity and sufficiency, and transgenerational avoidance assays

    PMID:38547071

    Open questions at the time
    • Whether other pathogens converge on maco-1 broadly unknown
    • Downstream consequences of maco-1 downregulation on neuronal physiology not measured
  7. 2025 Medium

    Positioned MACO-1 relative to the VAB-1 receptor within the avoidance circuit, showing VAB-1 loss reduces maco-1 expression and combined knockdown induces avoidance.

    Evidence RNAi knockdown, genetic epistasis, expression analysis, and behavioral avoidance assays

    PMID:40267186

    Open questions at the time
    • Placement inferred from expression-level changes, not direct biochemical interaction
    • Whether VAB-1 regulates maco-1 directly or indirectly unknown

Open questions

Synthesis pass · forward-looking unresolved questions
  • The biochemical activity of macoilin at the ER — its direct binding partners, the channels it assembles or traffics, and the molecular basis of its conserved neuronal function in mammals — remains undefined.
  • No identified direct physical substrate or interactor
  • No structural or domain-level mechanism
  • Mammalian (human MACO1) cellular function not characterized beyond ER localization

Mechanism profile

Synthesis pass · controlled-vocabulary classification · explore literature graph →
Localization
GO:0005783 endoplasmic reticulum 2
Pathway
R-HSA-112316 Neuronal System 2

Evidence

Reading pass · 8 per-paper findings extracted from the source corpus
Year Finding Method Journal Conf PMIDs
2011 MACO-1 (macoilin) is expressed broadly and specifically in the nervous system of C. elegans and localizes to the rough endoplasmic reticulum; it is excluded from dendrites and axons. Loss of maco-1 causes resistance to the cholinesterase inhibitor aldicarb and sensitivity to levamisole, indicating pre-synaptic defects. In maco-1 mutants, the O2-sensing neuron PQR fails to generate Ca2+ responses to rising O2, a defect that mirrors mutations in egl-19 (L-type voltage-gated Ca2+ channel α1 subunit), leading to the conclusion that macoilin acts in the ER to regulate assembly or trafficking of ion channels or ion channel regulators. Fluorescent protein localization, in vivo Ca2+ imaging, pharmacological assays (aldicarb/levamisole), genetic epistasis with egl-19/nca-1/nca-2 mutants PLoS genetics High 21437263
2011 Human macoilin (MACO1/TMEM57) and C. elegans MACO-1 both localize primarily to the rough endoplasmic reticulum. Expression of human macoilin in the C. elegans nervous system weakly rescues the thermotactic phenotype of maco-1 mutants, indicating functional conservation across species. maco-1 mutants show defective Ca2+ responses in AFD thermosensory neurons and AIY interneurons to thermal stimuli. Subcellular fractionation/localization, cross-species rescue by human MACO1 expression, in vivo Ca2+ imaging of AFD and AIY neurons PLoS genetics High 21589894
2017 MACO-1 functions downstream of the TIR-1/JNK-1 pathway to regulate forgetting of olfactory adaptation in C. elegans. Genetic screening identified maco-1 as a suppressor of the tir-1 gain-of-function excessive-forgetting phenotype. MACO-1 and the SCD-2/HEN-1 receptor tyrosine kinase–ligand pair act in parallel genetic pathways; only MACO-1 regulates forgetting of adaptation to isoamyl alcohol (sensed by different neuron types). Ca2+ imaging showed that odor-evoked Ca2+ response attenuation is sustained longer in maco-1 mutants, indicating that MACO-1 promotes recovery of sensory responses after conditioning. Forward genetic suppressor screen, double-mutant epistasis analysis, in vivo Ca2+ imaging, temporal neuronal silencing with histamine-gated chloride channels The Journal of neuroscience High 28924007
2016 maco-1 is required for pheromone-induced dauer formation in C. elegans, placing MACO-1 in the pathway for detection, transmission, or integration of ascaroside pheromone signals. Forward genetic screen (unbiased EMS mutagenesis), dauer formation assays G3 (Bethesda, Md.) Medium 26976437
2020 The C. elegans gene maco-1 is the target of P. aeruginosa PA14 non-coding small RNA P11; knockdown/loss of maco-1 is required for bacterially-induced pathogen avoidance behavior and its transgenerational inheritance. The RNAi and piRNA pathways, the germline, and the ASI neuron are all required for this behavior, placing maco-1 downstream of a trans-kingdom sRNA silencing pathway. Bacterial sRNA purification and feeding, RNAi knockdown, loss-of-function genetics, behavioral assays (avoidance), epistasis with RNAi/piRNA pathway mutants Nature High 32908307
2024 A P. vranovensis small RNA, Pv1, with 16-nt complementarity to an exon of C. elegans maco-1 is both necessary and sufficient to induce learned avoidance of P. vranovensis and its transgenerational inheritance, confirming that maco-1 downregulation by bacterial sRNAs is a conserved mechanism used by distinct Pseudomonas species. Bacterial sRNA sequencing, sRNA deletion and rescue (necessity/sufficiency), behavioral avoidance assays, transgenerational inheritance assays PLoS genetics High 38547071
2025 VAB-1 loss reduces maco-1 expression, and knockdown of both vab-1 and maco-1 induces P. fluorescens avoidance, placing both genes in the same bacterial sRNA-targeted pathogenic avoidance pathway. This genetic interaction places MACO-1 downstream of or parallel to VAB-1 in the avoidance circuit. RNAi knockdown, genetic epistasis, expression analysis, behavioral avoidance assays Science advances Medium 40267186
2002 The mouse orthologue of FLJ10747 (MACO1) shows slightly higher expression in testis relative to other tissues, and subcellular localization experiments indicate a strong nuclear localization, in contrast to SMP1 which is cytoplasmic. Tissue distribution analysis, subcellular localization by genomic/expression analysis of syntenic region Gene Low 12459264

Source papers

Stage 0 corpus · 17 papers · ranked by NIH iCite citations
Year Title Journal Citations PMID
2020 C. elegans interprets bacterial non-coding RNAs to learn pathogenic avoidance. Nature 165 32908307
2012 A genome-wide association scan on the levels of markers of inflammation in Sardinians reveals associations that underpin its complex regulation. PLoS genetics 130 22291609
2011 Implications of discoveries from genome-wide association studies in current cardiovascular practice. World journal of cardiology 60 21860704
2024 A natural bacterial pathogen of C. elegans uses a small RNA to induce transgenerational inheritance of learned avoidance. PLoS genetics 29 38547071
2011 Macoilin, a conserved nervous system-specific ER membrane protein that regulates neuronal excitability. PLoS genetics 26 21437263
2017 Multiple Signaling Pathways Coordinately Regulate Forgetting of Olfactory Adaptation through Control of Sensory Responses in Caenorhabditis elegans. The Journal of neuroscience : the official journal of the Society for Neuroscience 24 28924007
2016 A Forward Genetic Screen for Molecules Involved in Pheromone-Induced Dauer Formation in Caenorhabditis elegans. G3 (Bethesda, Md.) 15 26976437
2011 Novel and conserved protein macoilin is required for diverse neuronal functions in Caenorhabditis elegans. PLoS genetics 15 21589894
2014 Polymorphism of rs873308 near the transmembrane protein 57 gene is associated with serum lipid levels. Bioscience reports 14 27919029
2023 Astrocytes express aberrant immunoglobulins as putative gatekeeper of astrocytes to neuronal progenitor conversion. Cell death & disease 12 37015912
2025 Caenorhabditis Elegans as a Model for Environmental Epigenetics. Current environmental health reports 9 39828873
2002 Entire sequence of a mouse chromosomal segment containing the gene Rhced and a comparative analysis of the homologous human sequence. Gene 7 12459264
2013 Association of a complement receptor 1 gene variant with baseline erythrocyte sedimentation rate levels in patients starting anti-TNF therapy in a UK rheumatoid arthritis cohort: results from the Biologics in Rheumatoid Arthritis Genetics and Genomics Study Syndicate cohort. The pharmacogenomics journal 5 23856853
2018 An efficient analytic approach in genome-wide identification of methylation quantitative trait loci response to fenofibrate treatment. BMC proceedings 3 30275893
2025 C. elegans transgenerational avoidance of P. fluorescens is mediated by the Pfs1 sRNA and vab-1. Science advances 2 40267186
2024 Pseudomonas fluorescens 15 small RNA Pfs1 mediates transgenerational epigenetic inheritance of pathogen avoidance in C. elegans through the Ephrin receptor VAB-1. bioRxiv : the preprint server for biology 2 38826453
2023 A natural bacterial pathogen of C. elegans uses a small RNA to induce transgenerational inheritance of learned avoidance. bioRxiv : the preprint server for biology 1 37503135

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